s0byvy6

Property	Value
?:abstract	BACKGROUND: Severe acute respiratory syndrome-coronavirus-2 (SARS-CoV-2) infection causes direct lung damage, overwhelming endothelial activation, and inflammatory reaction, leading to acute respiratory failure and multi-organ dysfunction. Ongoing clinical trials are evaluating targeted therapies to hinder this exaggerated inflammatory response. Critically ill coronavirus disease 2019 (COVID-19) patients have shown heterogeneous severity trajectories, suggesting that response to therapies is likely to vary across patients. RESEARCH QUESTION: Are critically ill COVID-19 patients biologically and immunologically dissociable based on profiling of currently evaluated therapeutic targets? STUDY DESIGN AND METHODS: We did a single-center, prospective study in an ICU department in France. Ninety-six critically ill adult patients admitted with a documented SARS-CoV-2 infection were enrolled. We conducted principal components analysis and hierarchical clustering on a vast array of immunologic variables measured on the day of ICU admission. RESULTS: We found that patients were distributed in three clusters bearing distinct immunologic features and associated with different ICU outcomes. Cluster 1 had a “humoral immunodeficiency” phenotype with predominant B-lymphocyte defect, relative hypogammaglobulinemia, and moderate inflammation. Cluster 2 had a “hyperinflammatory” phenotype, with high cytokine levels (IL-6, IL-1β, IL-8, tumor necrosis factor-alpha [TNF⍺]) associated with CD4+ and CD8+ T-lymphocyte defects. Cluster 3 had a “complement-dependent” phenotype with terminal complement activation markers (elevated C3 and sC5b-9). INTERPRETATION: Patients with severe COVID-19 exhibiting cytokine release marks, complement activation, or B-lymphocyte defects are distinct from each other. Such immunologic variability argues in favor of targeting different mediators in different groups of patients and could serve as a basis for patient identification and clinical trial eligibility.
is ?:annotates of	<https://research.tib.eu/covid-19/entity/6s0byvy6_hasAnnotation_C0021368> <https://research.tib.eu/covid-19/entity/6s0byvy6_hasAnnotation_C0349410> <https://research.tib.eu/covid-19/entity/6s0byvy6_hasAnnotation_C1155266> <https://research.tib.eu/covid-19/entity/6s0byvy6_hasAnnotation_C1874451> <https://research.tib.eu/covid-19/entity/6s0byvy6_hasAnnotation_C5203676>
?:creator	<https://research.tib.eu/covid-19/entity/Dupont%2C_Thibault%3B_Caillat-Zucman%2C_Sophie%3B_Fremeaux-Bacchi%2C_V%C3%A9ronique%3B_Morin%2C_Florence%3B_Lenglin%C3%A9%2C_Etienne%3B_Darmon%2C_Michael%3B_Peffault_de_Latour%2C_R%C3%A9gis%3B_Zafrani%2C_Lara%3B_Azoulay%2C_Elie%3B_Dumas%2C_Guillaume>
?:doi	<https://research.tib.eu/covid-19/entity/10.1016/j.chest.2020.11.049>
?:doi	10.1016/j.chest.2020.11.049
?:journal	Chest
?:license	no-cc
?:pdf_json_files	document_parses/pdf_json/301bd099dc989533e3fc7988d06fd9b7c239d85a.json
?:pmc_json_files	document_parses/pmc_json/PMC7831685.xml.json
?:pmcid	<https://research.tib.eu/covid-19/entity/PMC7831685>
?:pmid	<https://research.tib.eu/covid-19/entity/33316234.0>
?:pmid	33316234.0
?:publication_isRelatedTo_Disease	<https://research.tib.eu/covid-19/entity/COVID-19>
is ?:relation_isRelatedTo_publication of	<https://research.tib.eu/covid-19/entity/6s0byvy6_HAS_C0021368_CAUSES_C0264490>
?:sha_id	<https://research.tib.eu/covid-19/entity/301bd099dc989533e3fc7988d06fd9b7c239d85a>
?:source	Elsevier; Medline; PMC
?:title	Identification of Distinct Immunophenotypes in Critically Ill Coronavirus Disease 2019 Patients
?:type	<https://research.tib.eu/covid-19/vocab/Publication>
?:year	2020-12-11

Property

Value

?:abstract

BACKGROUND: Severe acute respiratory syndrome-coronavirus-2 (SARS-CoV-2) infection causes direct lung damage, overwhelming endothelial activation, and inflammatory reaction, leading to acute respiratory failure and multi-organ dysfunction. Ongoing clinical trials are evaluating targeted therapies to hinder this exaggerated inflammatory response. Critically ill coronavirus disease 2019 (COVID-19) patients have shown heterogeneous severity trajectories, suggesting that response to therapies is likely to vary across patients. RESEARCH QUESTION: Are critically ill COVID-19 patients biologically and immunologically dissociable based on profiling of currently evaluated therapeutic targets? STUDY DESIGN AND METHODS: We did a single-center, prospective study in an ICU department in France. Ninety-six critically ill adult patients admitted with a documented SARS-CoV-2 infection were enrolled. We conducted principal components analysis and hierarchical clustering on a vast array of immunologic variables measured on the day of ICU admission. RESULTS: We found that patients were distributed in three clusters bearing distinct immunologic features and associated with different ICU outcomes. Cluster 1 had a “humoral immunodeficiency” phenotype with predominant B-lymphocyte defect, relative hypogammaglobulinemia, and moderate inflammation. Cluster 2 had a “hyperinflammatory” phenotype, with high cytokine levels (IL-6, IL-1β, IL-8, tumor necrosis factor-alpha [TNF⍺]) associated with CD4+ and CD8+ T-lymphocyte defects. Cluster 3 had a “complement-dependent” phenotype with terminal complement activation markers (elevated C3 and sC5b-9). INTERPRETATION: Patients with severe COVID-19 exhibiting cytokine release marks, complement activation, or B-lymphocyte defects are distinct from each other. Such immunologic variability argues in favor of targeting different mediators in different groups of patients and could serve as a basis for patient identification and clinical trial eligibility.

is ?:annotates of